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AB50843

Anti-Mitofusin 2 抗体

Anti-Mitofusin 2 antibody

4

(5 Reviews)

|

(19 Publications)

Rabbit Polyclonal Mitofusin 2 antibody. Suitable for WB and reacts with Mouse, Rat samples. Cited in 19 publications. Immunogen corresponding to Synthetic Peptide within Human MFN2 aa 550-600 conjugated to Keyhole Limpet Haemocyanin.

別名を表示する

CPRP1, KIAA0214, MFN2, Mitofusin-2, Transmembrane GTPase MFN2

2 Images
Western blot - Anti-Mitofusin 2 antibody (AB50843)
  • WB

Unknown

Western blot - Anti-Mitofusin 2 antibody (AB50843)

All lanes:

Western blot - Anti-Mitofusin 2 antibody (ab50843) at 0.25 µg/mL

Lane 1:

Rat brain mitochondria

Lane 2:

Mouse brain mitochondria

Secondary

All lanes:

Goat Anti-Rabbit IgG, Peroxidase conjugate and a chemiluminescent substrate.

Predicted band size: 86 kDa

Observed band size: 86 kDa

false

Western blot - Anti-Mitofusin 2 antibody (AB50843)
  • WB

CiteAb

Western blot - Anti-Mitofusin 2 antibody (AB50843)

Mitofusin 2 western blot using anti-Mitofusin 2 antibody ab50843. Publication image and figure legend from Ruiz, L., Salazar, C., et al., 2015, Oxid Med Cell Longev, PubMed 26106459.

ab50843 was used in this publication in western blot. This may not be the same as the application(s) guaranteed by Abcam. For a full list of applications guaranteed by Abcam for ab50843 please see the product overview.

Effect of quercetin treatment on the expression of PGC-1α, Mitofusin 2, VDAC, and protein oxidation. (a) Detection of carbonyl groups was performed with the OxyBlot Protein Oxidation Detection Kit. (c) Densitometry quantification of carbonyl groups was made with the ImageJ software. Carbonylation of proteins was normalized by Ponceau staining and Complex V (CV) expression. (b) Expression of mitochondrial proteins. Protein expression of MFN2, PGC-1α, and VDAC1 was analyzed in heart isolated mitochondria from control and quercetin-treated mice. β-actin was used as a loading control. (d) Densitometry analysis. MFN2, PGC-1α, and VDAC1 expressions were normalized by β-actin expression. Each bar represents the mean ± SD, analyzed by two-sample t-test (P < 0.05). Control mice, n = 11; quercetin-treated mice, n = 9. Each bar represents the mean ± SD, analyzed by two-sample t-test (P < 0.05). Significant differences (*) were found between control and quercetin-treated mice. P < 0.05.

false

Key facts

宿主種

Rabbit

クローン性

Polyclonal

アイソタイプ

IgG

キャリアフリー

No

交差種

Mouse, Rat

アプリケーション

WB

applications

免疫原

Synthetic Peptide within Human MFN2 aa 550-600 conjugated to Keyhole Limpet Haemocyanin. The exact immunogen used to generate this antibody is proprietary information.

O95140

Reactivity data

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AB124773

Anti-Mitofusin 2 antibody [NIAR164]

4
6 Reviews
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出荷温度及び保存条件

製品の状態
Liquid
精製方法
Affinity purification Immunogen
バッファー組成
pH: 7.4 Preservative: 0.097% Sodium azide Constituents: 0.0268% PBS
出荷温度
Blue Ice
短期保存期間
1-2 weeks
短期保存温度
+4°C
長期保存温度
-20°C
分注に関する情報
Upon delivery aliquot
保管に関する情報
Avoid freeze / thaw cycle

補足情報

This supplementary information is collated from multiple sources and compiled automatically.

Mitofusin 2 also known as MFN2 is a protein involved in the regulation of mitochondrial fusion. The MFN2 molecular weight is roughly 86 kDa. It plays an important role in connecting and merging the outer membranes of mitochondria which is vital for maintaining mitochondrial function and integrity. Mitofusin 2 proteins are expressed in many tissues but they are abundantly present in energy-demanding tissues like skeletal muscle heart and the brain.
Biological function summary

Mitofusin 2 ensures the proper distribution of mitochondria within cells and regulates mitochondrial metabolism. It is a critical component of the mitochondrial fusion machinery and works closely with its homolog Mitofusin 1 (MFN1). Together they form a complex that facilitates the physical merging of mitochondrial membranes. This process is essential for mitochondrial dynamics which include not only fusion but also fission and biogenesis.

Pathways

The protein part of the fusion machinery integrates into multiple essential biological pathways including energy metabolism and apoptosis regulation. It participates in the mitochondrial fusion pathway and the PGC-1α pathway for mitochondrial biogenesis. Mitofusin 2 interacts with proteins such as PINK1 and Parkin that are known to play roles in mitophagy a process that targets damaged mitochondria for degradation indicating its involvement in maintaining mitochondrial quality control.

Mutations in Mitofusin 2 have been linked to Charcot-Marie-Tooth disease type 2A (CMT2A) a neuropathy that affects peripheral nerves. This protein also shows connections to metabolic disorders such as obesity and type 2 diabetes. In these conditions its interaction with other proteins like OPA1 involved in mitochondrial inner membrane fusion influences mitochondrial dysfunction a recognized feature contributing to disease pathogenesis. Understanding MFN2's function and role in disease can help develop targeted therapies for these conditions.

製品プロトコール

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ターゲットの情報

Mitochondrial outer membrane GTPase that mediates mitochondrial clustering and fusion (PubMed : 11181170, PubMed : 11950885, PubMed : 19889647, PubMed : 26214738, PubMed : 28114303). Mitochondria are highly dynamic organelles, and their morphology is determined by the equilibrium between mitochondrial fusion and fission events (PubMed : 28114303). Overexpression induces the formation of mitochondrial networks (PubMed : 28114303). Membrane clustering requires GTPase activity and may involve a major rearrangement of the coiled coil domains (Probable). Plays a central role in mitochondrial metabolism and may be associated with obesity and/or apoptosis processes (By similarity). Plays an important role in the regulation of vascular smooth muscle cell proliferation (By similarity). Involved in the clearance of damaged mitochondria via selective autophagy (mitophagy) (PubMed : 23620051). Is required for PRKN recruitment to dysfunctional mitochondria (PubMed : 23620051). Involved in the control of unfolded protein response (UPR) upon ER stress including activation of apoptosis and autophagy during ER stress (By similarity). Acts as an upstream regulator of EIF2AK3 and suppresses EIF2AK3 activation under basal conditions (By similarity).
See full target information MFN2

文献 (19)

Recent publications for all applications. Explore the full list and refine your search

International journal of molecular sciences 24: PubMed37834400

2023

Diaphragm Fatigue in SMNΔ7 Mice and Its Molecular Determinants: An Underestimated Issue.

Applications

Unspecified application

Species

Unspecified reactive species

Francesca Cadile,Deborah Recchia,Massimiliano Ansaldo,Paola Rossi,Giorgia Rastelli,Simona Boncompagni,Lorenza Brocca,Maria Antonietta Pellegrino,Monica Canepari

Basic research in cardiology 118:20 PubMed37212935

2023

SMYD1a protects the heart from ischemic injury by regulating OPA1-mediated cristae remodeling and supercomplex formation.

Applications

Unspecified application

Species

Unspecified reactive species

Marta W Szulik,Steven Valdez,Maureen Walsh,Kathryn Davis,Ryan Bia,Emilee Horiuchi,Sean O'Very,Anil K Laxman,Linda Sandaklie-Nicolova,David R Eberhardt,Jessica R Durrant,Hanin Sheikh,Samuel Hickenlooper,Magnus Creed,Cameron Brady,Mickey Miller,Li Wang,June Garcia-Llana,Christopher Tracy,Stavros G Drakos,Katsuhiko Funai,Dipayan Chaudhuri,Sihem Boudina,Sarah Franklin

Frontiers in cell and developmental biology 11:1145182 PubMed37091980

2023

The bisphenol S contamination level observed in human follicular fluid affects the development of porcine oocytes.

Applications

Unspecified application

Species

Unspecified reactive species

Tereza Žalmanová,Kristýna Hošková,Šárka Prokešová,Jan Nevoral,Michal Ješeta,Michal Benc,Young-Joo Yi,Jiří Moravec,Beáta Močáryová,Stanislava Martínková,Josef Fontana,Moustafa Elkalaf,Jan Trnka,Jana Žáková,Jaroslav Petr

Cells 11: PubMed35805195

2022

Activation of Autophagic Flux Maintains Mitochondrial Homeostasis during Cardiac Ischemia/Reperfusion Injury.

Applications

Unspecified application

Species

Unspecified reactive species

Lihao He,Yuxin Chu,Jing Yang,Jin He,Yutao Hua,Yunxi Chen,Gloria Benavides,Glenn C Rowe,Lufang Zhou,Scott Ballinger,Victor Darley-Usmar,Martin E Young,Sumanth D Prabhu,Palaniappan Sethu,Yingling Zhou,Cheng Zhang,Min Xie

Journal of applied physiology (Bethesda, Md. : 1985) 133:191-204 PubMed35678745

2022

Mitochondrial adaptations to inactivity in diaphragm muscle fibers.

Applications

Unspecified application

Species

Unspecified reactive species

Alyssa D Brown,Matthew J Fogarty,Leah A Davis,Debanjali Dasgupta,Carlos B Mantilla,Gary C Sieck

The Journal of physiology 599:4337-4356 PubMed34368970

2021

Predominant cause of faster force recovery in females than males after intense eccentric contractions in mouse fast-twitch muscle.

Applications

Unspecified application

Species

Unspecified reactive species

Daiki Watanabe,Ryo Ikegami,Yutaka Kano

BMB reports 54:305-310 PubMed33408001

2021

Long-term depletion of cereblon induces mitochondrial dysfunction in cancer cells.

Applications

Unspecified application

Species

Unspecified reactive species

Seulki Park,Kidae Kim,Keeok Haam,Hyun Seung Ban,Jung-Ae Kim,Byoung Chul Park,Sung Goo Park,Sunhong Kim,Jeong-Hoon Kim

American journal of physiology. Lung cellular and molecular physiology 320:L137-L151 PubMed33146568

2020

TNFα induces mitochondrial fragmentation and biogenesis in human airway smooth muscle.

Applications

Unspecified application

Species

Unspecified reactive species

Philippe Delmotte,Natalia Marin Mathieu,Gary C Sieck

International journal of biological sciences 16:2788-2802 PubMed33061796

2020

Deletion of Mitochondrial Uncoupling Protein 2 Exacerbates Mitochondrial Damage in Mice Subjected to Cerebral Ischemia and Reperfusion Injury under both Normo- and Hyperglycemic Conditions.

Applications

Unspecified application

Species

Unspecified reactive species

Maotao He,Yanmei Ma,Rui Wang,Jianzhong Zhang,Li Jing,P Andy Li

Journal of dermatological science 99:109-118 PubMed32636049

2020

Loss of dynamin-related protein 1 (Drp1) does not affect epidermal development or UVB-induced apoptosis but does accelerate UVB-induced carcinogenesis.

Applications

Unspecified application

Species

Unspecified reactive species

Teruki Yanagi,Shinya Kitamura,Keisuke Imafuku,Asuka Suto,Takuya Maeda,Shinya Tanaka,Hiromi Sesaki,Riichiro Abe,Hiroshi Shimizu
View all publications

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